Interplay between chromosomal alterations and gene mutations shapes the evolutionary trajectory of clonal hematopoiesis

Author:

Gao TengORCID,Ptashkin Ryan,Bolton Kelly L.,Sirenko MariaORCID,Fong Christopher,Spitzer Barbara,Menghrajani Kamal,Ossa Juan E. Arango,Zhou Yangyu,Bernard ElsaORCID,Levine MaxORCID,Martinez Juan S. Medina,Zhang Yanming,Franch-Expósito SebastiàORCID,Patel Minal,Braunstein Lior Z.,Kelly Daniel,Yabe Mariko,Benayed RymaORCID,Caltabellotta Nicole M.,Philip JohnORCID,Paraiso Ederlinda,Mantha Simon,Solit David B.ORCID,Diaz Luis A.,Berger Michael F.ORCID,Klimek Virginia,Levine Ross L.ORCID,Zehir AhmetORCID,Devlin Sean M.,Papaemmanuil ElliORCID

Abstract

AbstractStably acquired mutations in hematopoietic cells represent substrates of selection that may lead to clonal hematopoiesis (CH), a common state in cancer patients that is associated with a heightened risk of leukemia development. Owing to technical and sample size limitations, most CH studies have characterized gene mutations or mosaic chromosomal alterations (mCAs) individually. Here we leverage peripheral blood sequencing data from 32,442 cancer patients to jointly characterize gene mutations (n = 14,789) and mCAs (n = 383) in CH. Recurrent composite genotypes resembling known genetic interactions in leukemia genomes underlie 23% of all detected autosomal alterations, indicating that these selection mechanisms are operative early in clonal evolution. CH with composite genotypes defines a patient group at high risk of leukemia progression (3-year cumulative incidence 14.6%, CI: 7–22%). Multivariable analysis identifies mCA as an independent risk factor for leukemia development (HR = 14, 95% CI: 6–33, P < 0.001). Our results suggest that mCA should be considered in conjunction with gene mutations in the surveillance of patients at risk of hematologic neoplasms.

Funder

U.S. Department of Health & Human Services | NIH | National Cancer Institute

V Foundation for Cancer Research

Damon Runyon Cancer Research Foundation

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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